Rex J H, Aronson B D, Somerville R L
Department of Biochemistry, Purdue University, West Lafayette, Indiana 47907.
J Bacteriol. 1991 Oct;173(19):5944-53. doi: 10.1128/jb.173.19.5944-5953.1991.
The tdh promoter of Escherichia coli is induced seven- to eightfold when cells are grown in the presence of exogenous leucine. A scheme was devised to select mutants that exhibited high constitutive expression of the tdh promoter. The mutations in these strains were shown to lie within a previously identified gene (lrp) that encodes Lrp (leucine-responsive regulatory protein). By deletion analysis, the site of action of Lrp was localized to a 25-bp region between coordinates -69 and -44 of the tdh promoter. Disruption of a 12-bp presumptive target sequence found in this region of tdh resulted in constitutively derepressed expression from the tdh promoter. Similar DNA segments (consensus, TTTATTCtNaAT) were also identified in a number of other promoters, including each of the Lrp-regulated promoters whose nucleotide sequence is known. The sequence of the promoter region of serA, an Lrp-regulated gene, was determined. No Lrp consensus target sequence was present upstream of serA, suggesting that Lrp acts indirectly on the serA promoter. A previously described mutation in a leucine-responsive trans-acting factor, LivR (J. J. Anderson, S. C. Quay, and D. L. Oxender, J. Bacteriol. 126:80-90, 1976), resulted in constitutively repressed expression from the tdh promoter and constitutively induced expression from the serA promoter. The possibility that LivR and Lrp are allelic is discussed.
当细胞在外源亮氨酸存在的情况下生长时,大肠杆菌的tdh启动子会被诱导7至8倍。设计了一个方案来筛选表现出tdh启动子高组成型表达的突变体。这些菌株中的突变被证明位于先前鉴定的编码Lrp(亮氨酸响应调节蛋白)的基因(lrp)内。通过缺失分析,Lrp的作用位点被定位到tdh启动子坐标-69至-44之间的一个25bp区域。破坏在tdh的该区域中发现的一个12bp推定靶序列导致tdh启动子组成型去阻遏表达。在许多其他启动子中也鉴定到了类似的DNA片段(共有序列,TTTATTCtNaAT),包括其核苷酸序列已知的每个Lrp调节的启动子。测定了Lrp调节基因serA的启动子区域序列。在serA上游不存在Lrp共有靶序列,这表明Lrp间接作用于serA启动子。先前描述的亮氨酸响应反式作用因子LivR中的一个突变(J. J. Anderson、S. C. Quay和D. L. Oxender,《细菌学杂志》126:80 - 90,1976)导致tdh启动子组成型阻遏表达和serA启动子组成型诱导表达。讨论了LivR和Lrp是等位基因的可能性。